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Melanoma patient-derived xenografts accurately model the disease and develop fast enough to guide treatment decisions

机译:黑色素瘤患者来源的异种移植物可以准确地对疾病进行建模并发展得足够快以指导治疗决策

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摘要

The development of novel therapies against melanoma would benefit from individualized tumor models to ensure the rapid and accurate identification of biomarkers of therapy response. Previous studies have suggested that patient-derived xenografts (PDXes) could be useful. However, the utility of PDXes in guiding real-time treatment decisions has only been reported in anecdotal forms. Here tumor biopsies from patients with stage III and IV metastatic malignant melanoma were transplanted into immunocompromised mice to generate PDXes. 23/26 melanoma biopsies generated serially transplantable PDX models, and their histology, mutation status and expression profile resembled their corresponding patient biopsy. The potential treatment for one patient was revealed by an in vitro drug screen and treating PDXes with the MEK inhibitor trametinib. In another patient, the BRAF mutation predicted the response of both the patient and its corresponding PDXes to MAPK-targeted therapy. Importantly, in this unselected group of patients, the time from biopsy for generation of PDXes until death was significantly longer than the time required to reach the treatment phase of the PDXes. Thus, it could be clinically meaningful to use this type of platform for melanoma patients as a pre-selection tool in clinical trials.
机译:针对黑素瘤的新疗法的发展将受益于个性化的肿瘤模型,以确保快速准确地确定治疗反应的生物标志物。先前的研究表明,患者来源的异种移植物(PDXes)可能有用。但是,PDX在指导实时治疗决策中的效用仅以传闻形式报道。在这里,来自III期和IV期转移性恶性黑色素瘤患者的肿瘤活检被移植到免疫功能低下的小鼠中以产生PDXes。 23/26黑色素瘤活检产生了可串行移植的PDX模型,其组织学,突变状态和表达谱与相应的患者活检相似。通过体外药物筛选并用MEK抑制剂曲美替尼治疗PDXes,揭示了一名患者的潜在治疗方法。在另一位患者中,BRAF突变预测了患者及其相应的PDXes对MAPK靶向治疗的反应。重要的是,在这一非选择的患者组中,从活检产生PDXes到死亡的时间明显长于达到PDXes治疗阶段所需的时间。因此,将这种类型的黑色素瘤患者平台用作临床试验中的预选工具可能具有临床意义。

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